First study of oncolytic HSV-1 in children & young adults with cancer indicates safety and tolerability

HSV1716 – an oncolytic herpes simplex virus-1 – has been studied in adults via injection into the brain and superficial tumours.

Now, a team of researchers at Nationwide Children’s Hospital and Cincinnati Children’s Hospital Medical Center have completed the first phase 1 trial of the virus in the paediatric population, published online in Clinical Cancer Research.

Children with relapsed or refractory solid tumours continue to have poor outcomes and significant toxicities from available therapies.

Researchers and clinicians are looking to novel strategies and treatments to improve those outcomes – including oncolytic virotherapy, which has shown improved outcomes and decreased toxicities in numerous adult and animal studies.

“The virus we tested — HSV1716 — is similar to talimogene laherparepvec, the HSV-1 recently FDA-approved for melanoma by intralesional injection,” says Timothy Cripe, MD, PhD, division chief of Haematology/Oncology & BMT, principal investigator in the Center for Childhood Cancer and Blood Diseases in The Research Institute at Nationwide Children’s and senior author on the study. “Oncolytic viruses have a high potential for therapeutic performance with limited toxic effects due to their tumour-selective attributes.”

The researchers administered a single dose of HSV1716 to eight trial participants and two doses to one participant.

The participants ranged in age from 8 to 30 years, and their diagnoses included a variety of sarcomas, clival chordoma, malignant peripheral nerve sheath tumour (MPNST) and renal cell carcinoma.

No dose-limiting toxicities were observed in any of the participants.

All adverse events reported that were likely to be related to the virus or the procedure were mild and transient.

No clinical responses were observed in this early safety study.

However, the results are promising for future investigations into optimal virus dosing, method of virus delivery and combination therapy with other cancer treatments, including chemotherapy and immunomodulators, according to Dr. Cripe.

“We observed that intratumoral HSV1716 is safe and well-tolerated without shedding in children and young adults with late-stage, aggressive cancer,” says Dr. Cripe, who is also professor of Paediatrics at The Ohio State University College of Medicine. “We also observed viremia consistent with viral replication and transient inflammatory reactions, both of which indicate promise for future studies.”